PMID- 29372930
OWN - NLM
STAT- MEDLINE
DCOM- 20180301
LR  - 20220801
IS  - 1469-493X (Electronic)
IS  - 1361-6137 (Linking)
VI  - 1
IP  - 1
DP  - 2018 Jan 16
TI  - Eliciting adverse effects data from participants in clinical trials.
PG  - MR000039
LID - 10.1002/14651858.MR000039.pub2 [doi]
LID - MR000039
AB  - BACKGROUND: Analysis of drug safety in clinical trials involves assessing adverse 
      events (AEs) individually or by aggregate statistical synthesis to provide 
      evidence of likely adverse drug reactions (ADR). While some AEs may be 
      ascertained from physical examinations or tests, there is great reliance on 
      reports from participants to detect subjective symptoms, where he/she is often 
      the only source of information. There is no consensus on how these reports should 
      be elicited, although it is known that questioning methods influence the extent 
      and nature of data detected. This leaves room for measurement error and 
      undermines comparisons between studies and pooled analyses. This review 
      investigated comparisons of methods used in trials to elicit participant-reported 
      AEs. This should contribute to knowledge about the methodological challenges and 
      possible solutions for achieving better, or more consistent, AE ascertainment in 
      trials. OBJECTIVES: To systematically review the research that has compared 
      methods used within clinical drug trials (or methods that would be specific for 
      such trials) to elicit information about AEs defined in the protocol or in the 
      planning for the trial. SEARCH METHODS: Databases (searched to March 2015 unless 
      indicated otherwise) included: Embase; MEDLINE; MEDLINE in Process and Other 
      Non-Indexed Citations; Cochrane Methodology Register (July 2012); Cochrane 
      Central Register of Controlled Trials (February 2015); Cochrane Database of 
      Systematic Reviews; Database of Abstracts of Reviews of Effects (January 2015); 
      Health Technology Assessment database (January 2015); CINAHL; CAB Abstracts; 
      BIOSIS (July 2013); Science Citation Index; Social Science Citation Index; 
      Conference Proceedings Citation Index - Science. The search used thesaurus 
      headings and synonyms for the following concepts: (A): Adverse events AND 
      measurement; (B): Participants AND elicitation (also other synonyms for 
      extraction of information about adverse effects from people); (C): Participants 
      AND checklists (also other synonyms as for B). Pragmatic ways were used to limit 
      the results whilst trying to maintain sensitivity. There were no date or sample 
      size restrictions but only reports published in English were included fully, 
      because of resource constraints as regards translation. SELECTION CRITERIA: Two 
      types of studies were included: drug trials comparing two or more methods within- 
      or between-participants to elicit participant-reported AEs, and research studies 
      performed outside the context of a trial to compare methods which could be used 
      in trials (evidenced by reference to such applicability). Primary outcome data 
      included AEs elicited from participants taking part in any such clinical trial. 
      We included any participant-reported data relevant for an assessment of 
      drug-related harm, using the original authors' terminology (and definition, where 
      available), with comment on whether the data were likely to be treatment-emergent 
      AEs or not. DATA COLLECTION AND ANALYSIS: Titles and abstracts were independently 
      reviewed for eligibility. Full texts of potentially eligible citations were 
      independently reviewed for final eligibility. Relevant data were extracted and 
      subjected to a 100% check. Disagreements were resolved by discussion, involving a 
      third author. The risk of bias was independently assessed by two authors. The 
      Cochrane 'Risk of bias' tool was used for reports comparing outcomes between 
      participants, while for within-participant comparisons, each study was critically 
      evaluated in terms of potential impact of the design and conduct on findings 
      using the framework of selection, performance, detection, attrition, reporting, 
      and other biases. An attempt was made to contact authors to retrieve protocols or 
      specific relevant missing information. Reports were not excluded on the basis of 
      quality unless data for outcomes were impossible to compare (e.g. where 
      denominators differed). A narrative synthesis was conducted because differences 
      in study design and presentation meant that a quantitative meta-analysis was not 
      possible. MAIN RESULTS: The 33 eligible studies largely compared open questions 
      with checklist-type questions or rating scales. Two included participant 
      interviews. Despite different designs, populations and details of questioning 
      methods, the narrative review showed that more specific questioning of 
      participants led to more AEs detected compared to a more general enquiry. A 
      subset of six studies suggested that more severe, bothersome, or otherwise 
      clinically relevant AEs were reported when an initial open enquiry was used, 
      while some less severe, bothersome, or clinically relevant AEs were only reported 
      with a subsequent specific enquiry. However, two studies showed that quite severe 
      or debilitating AEs were only detected by an interview, while other studies did 
      not find a difference in the nature of AEs between elicitation methods. No 
      conclusions could be made regarding the impact of question method on the ability 
      to detect a statistically significant difference between study groups. There was 
      no common statistical rubric, but we were able to represent some effect measures 
      as a risk ratio of the proportion of participants with at least one AE. This 
      showed a lower level of reporting for open questions (O) compared to checklists 
      (CL), with a range for the risk ratios of 0.12 to 0.64. AUTHORS' CONCLUSIONS: 
      This review supports concerns that methods to elicit participant-reported AEs 
      influence the detection of these data. There was a risk for under-detection of 
      AEs in studies using a more general elicitation method compared to those using a 
      comprehensive method. These AEs may be important from a clinical perspective or 
      for patients. This under-detection could compromise ability to pool AE data. 
      However, the impact on the nature of the AE detected by different methods is 
      unclear. The wide variety and low quality of methods to compare elicitation 
      strategies limited this review. Future studies would be improved by using and 
      reporting clear definitions and terminology for AEs (and other important 
      variables), frequency and time period over which they were ascertained, how they 
      were graded, assessed for a relationship to the study drug, coded, and 
      tabulated/reported. While the many potential AE endpoints in a trial may preclude 
      the development of general AE patient-reported outcome measurement instruments, 
      much could also be learnt from how these employ both quantitative and qualitative 
      methods to better understand data elicited. Any chosen questioning method needs 
      to be feasible for use by both staff and participants.
FAU - Allen, Elizabeth N
AU  - Allen EN
AD  - Division of Clinical Pharmacology, Department of Medicine, University of Cape 
      Town, K45, Old Main Building, Groote Schuur Hospital, Observatory, Cape Town, 
      Western Cape, South Africa, 7925.
FAU - Chandler, Clare Ir
AU  - Chandler CI
FAU - Mandimika, Nyaradzo
AU  - Mandimika N
FAU - Leisegang, Cordelia
AU  - Leisegang C
FAU - Barnes, Karen
AU  - Barnes K
LA  - eng
PT  - Journal Article
PT  - Research Support, Non-U.S. Gov't
PT  - Review
PT  - Systematic Review
DEP - 20180116
PL  - England
TA  - Cochrane Database Syst Rev
JT  - The Cochrane database of systematic reviews
JID - 100909747
SB  - IM
UOF - doi: 10.1002/14651858.MR000039
MH  - *Checklist
MH  - *Clinical Trials as Topic
MH  - *Drug-Related Side Effects and Adverse Reactions
MH  - Humans
MH  - *Research Subjects
PMC - PMC7098080
COIS- The review authors have no interests to declare.
EDAT- 2018/01/27 06:00
MHDA- 2018/03/02 06:00
PMCR- 2019/01/16
CRDT- 2018/01/27 06:00
PHST- 2018/01/27 06:00 [pubmed]
PHST- 2018/03/02 06:00 [medline]
PHST- 2018/01/27 06:00 [entrez]
PHST- 2019/01/16 00:00 [pmc-release]
AID - MR000039.pub2 [pii]
AID - 10.1002/14651858.MR000039.pub2 [doi]
PST - epublish
SO  - Cochrane Database Syst Rev. 2018 Jan 16;1(1):MR000039. doi: 
      10.1002/14651858.MR000039.pub2.